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The Nobel Prize in Physiology or Medicine 1985

The Nobel Prize in Physiology or Medicine 1985. for their discoveries concerning "the regulation of cholesterol metabolism”. Michal S. Brown. Joseph L.Goldstein. University of Texas Southwestern Medical Center at Dallas Dallas, TX, USA. The Nobel Prize in Physiology or Medicine 1985.

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The Nobel Prize in Physiology or Medicine 1985

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  1. The Nobel Prize in Physiology or Medicine 1985

  2. for their discoveries concerning "the regulation of cholesterol metabolism” Michal S. Brown Joseph L.Goldstein University of Texas Southwestern Medical Center at Dallas Dallas, TX, USA

  3. The Nobel Prize in Physiology or Medicine 1985 • Cells on their surfaces have receptors which mediate the uptake of the cholesterol-containing particles called LDL(low-density lipoprotein) that circulate in the blood stream. • Underlying mechanism to the severe hereditary familial hypercholesterolemia is a complete, or partial, lack of functional LDL-receptors.

  4. Cholesterol – an important substance • Originates from two main sources -Biosynthesis in the liver -Fat from the food • Two main functions : structural component in cell membranes and is converted to certain steroid hormones(testosteron, cortison , estrogen and aldactone) and bile salts. • Vitamin D

  5. Cholesterol packeted into particles called lipoprotein-a combination of fat and proteins.

  6. Figure 1. The LDL is a spherical particle with a radius of one millionth millimeter. Most of the cholesterol in the blood stream is found in LDL particles. Its core consists of approximately 1,500 cholesteryl esters, each a cholesterol molecule attached by an ester linkage to a long fatty acid chain. The core is surrounded by a surface coat composed of 800 molecules of phospholipid, 500 molecules of unesterified cholesterol and one large protein molecule, apoprotein B, which moors the LDL to the receptor on the cell surface.

  7. The Nobel Prize in Physiology or Medicine 1985 • In normal individuals the uptake of dietary cholesterol inhibits the cells own synthesis of cholesterol. As a consequence the number of LDL-receptors on the cell surface is reduced. • This leads to increased levels of cholesterol in the blood which subsequently may accumulate in the wall of arteries causing atherosclerosis and eventually a heart attack or a stroke.

  8. Normal healthy person has 2g cholesterol per liter plasma. • Abnormal values approximately 10 g per liter. • Studies on patients with familial hypercholesterolemia (FH) by Brown and Goldstein constitute founding stones for our present knowledge concerning the cholesterol metablolism.

  9. Studies of Brown and Goldstein • Studied Cultured cells(fibroblasts) from healthy individuals and individuals with FH. • The fibroblasts from patients with the most severe form of FH completely lacked functional LDL-receptors whereas with milder form of FH has fewer LDL-receptors than normal

  10. Studies of Brown and Goldstein • Discovered that the synthesis of cholesterol in normal fibroblasts was inhibited when LDL-containing serum was added to the cell culture. • Fibroblasts from homozygous patients with FH were not inhibited since they lacked functional LDL-receptors. Consequently their intracellular synthesis could not be influenced.

  11. Studies of Brown and Goldstein • In later studies Brown and Goldstein showed that LDL which had bound to the receptor was taken up by the cells as a LDL-receptor complex.

  12. Receptor-mediated endocytosis

  13. LDL receptors, one healthy and two abnormal. The part of the receptor localized outside the cell membrane is identical in all three cases. The difference is found in the portion of the receptor inside the cell membrane

  14. Treatment of FH based on their discovery of the LDL-receptor • Treatment of FH based on their discovery of the LDL-receptor. • Milder heterozygous form of FH- the number of LDL-receptors has been increased using drugs- cholestyramine and mevinolin. • Severe homozygous form of FH, where functional LDL-receptors are missing, medication is no therapeutic alternative.

  15. References • http://nobelprize.org/nobel_prizes/medicine/laureates/1985/ • http://www8.utsouthwestern.edu/utsw/cda/dept14857/files/114532.html • http://www.americanheart.org/presenter.jhtml?identifier=4440

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